Your search keyword '"Afagh Alavi"' showing total 68 results

1. Potential role of FKBP5 single‐nucleotide polymorphisms in functional seizures

Author

Ali A. Asadi‐Pooya, Leila Simani, Marjan Asadollahi, Fatemeh Sadat Rashidi, Ehsan Ahmadipour, Afagh Alavi, Mehrdad Roozbeh, Nayyereh Akbari, and Negar Firouzabadi

Subjects

dissociative, genetic, nonepileptic, psychogenic, seizure, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Objective We investigated the associations between FKBP5 single‐nucleotide polymorphisms (SNPs) and functional seizures (FS). Methods Seventy patients with FS, 140 with major depressive disorder (MDD), and 140 healthy controls were studied. Their DNAs were analyzed for the rs1360780 in the 3′ region and rs9470080 in the 5′ region of the FKBP5. Childhood trauma questionnaire and hospital anxiety and depression scale were used. Results Patients with FS and those with MDD had less GG and more AA genotypes in both rs9470080 and rs1360780 SNPs compared with those in healthy controls. Similar results were observed for allelic frequencies. There were no significant differences between FS and MDD groups in terms of genotype and allelic frequencies for both SNPs. The results of multinomial logistic regression analysis showed that FKBP5 polymorphisms were not associated with the diagnosis. Significance Patients with FS and those with MDD had significantly different genotypes in both rs9470080 and rs1360780 SNPs compared with those in healthy controls. However, it seems that FKBP5 polymorphisms were not associated with FS in the absence of depression. Further genetic investigations of patients with FS may increase our understanding of the neurobiological underpinnings of this condition, but such studies should be large enough and very well designed; they should include a comparison group with depression in addition to a healthy control group.

Published

2023

2. Intellectual disability associated with craniofacial dysmorphism due to POLR3B mutation and defect in spliceosomal machinery

Author

Mostafa Saghi, Kolsoum InanlooRahatloo, Afagh Alavi, Kimia Kahrizi, and Hossein Najmabadi

Subjects

Internal medicine, RC31-1245, Genetics, QH426-470

Abstract

Abstract Background Intellectual disability (ID) is a clinically important disease and a most prevalent neurodevelopmental disorder. The etiology and pathogenesis of ID are poorly recognized. Exome sequencing revealed a homozygous missense mutation in the POLR3B gene in a consanguineous family with three Intellectual disability with craniofacial anomalies patients. POLR3B gene encoding the second largest subunit of RNA polymerase III. Methods We performed RNA sequencing on blood samples to obtain insights into the biological pathways influenced by POLR3B mutation. We applied the results of our RNA-Seq analysis to several gene ontology programs such as ToppGene, Enrichr, KEGG. Results A significant decrease in expression of several spliceosomal RNAs, ribosomal proteins, and transcription factors was detected in the affected, compared to unaffected, family members. Conclusions We hypothesize that POLR3B mutation dysregulates the expression of some important transcription factors, ribosomal and spliceosomal genes, and impairments in protein synthesis and splicing mediated in part by transcription factors such as FOXC2 and GATA1 contribute to impaired neuronal function and concurrence of intellectual disability and craniofacial anomalies in our patients. Our study highlights the emerging role of the spliceosome and ribosomal proteins in intellectual disability.

Published

2022

3. Identification of let-7f and miR-338 as plasma-based biomarkers for sporadic amyotrophic lateral sclerosis using meta-analysis and empirical validation

Author

Narges Daneshafrooz, Mohammad Taghi Joghataei, Mehdi Mehdizadeh, Afagh Alavi, Mahmood Barati, Bahman Panahi, Shahram Teimourian, and Babak Zamani

Subjects

Medicine, Science

Abstract

Abstract Amyotrophic lateral sclerosis (ALS) is a lethal neurodegenerative disease that in most cases occurs sporadic (sALS). The disease is not curable, and its pathogenesis mechanisms are not well understood yet. Given the intricacy of underlying molecular interactions and heterogeneity of ALS, the discovery of molecules contributing to disease onset and progression will open a new avenue for advancement in early diagnosis and therapeutic intervention. Here we conducted a meta-analysis of 12 circulating miRNA profiling studies using the robust rank aggregation (RRA) method, followed by enrichment analysis and experimental verification. We identified miR-451a and let-7f-5p as meta-signature miRNAs whose targets are involved in critical pathogenic pathways underlying ALS, including ‘FoxO signaling pathway’, ‘MAPK signaling pathway’, and ‘apoptosis’. A systematic review of 7 circulating gene profiling studies elucidated that 241 genes up-regulated in sALS circulation with concomitant being targets of the meta-signature miRNAs. Protein–protein interaction (PPI) network analysis of the candidate targets using MCODE algorithm revealed the main subcluster is involved in multiple cascades eventually leads apoptosis, including ‘positive regulation of neuron apoptosis. Besides, we validated the meta-analysis results using RT-qPCR. Indeed, relative expression analysis verified let-7f-5p and miR-338-3p as significantly down-regulated and up-regulated biomarkers in the plasma of sALS patients, respectively. Receiver operating characteristic (ROC) analysis also highlighted the let-7f-5p and miR-338-3p potential as robustness plasma biomarkers for diagnosis and potential therapeutic targets of sALS disease.

Published

2022

4. An overview of Neurodegeneration with brain iron accumulation (NBIA) syndromes and the disease status in Iranian population: review article

Author

Reza Hajati, Mohammad Masoud Rahimi Bidgoli, Mohammad Rohani, and Afagh Alavi

Subjects

basal ganglia, genetic heterogeneity, iron metabolism disorders, neurodegeneration with brain iron accumulation (nbia), review, Medicine (General), R5-920

Abstract

Neurodegeneration with brain iron accumulation (NBIA) is a rare set of inherited neurodegenerative disorders with abnormal accumulation of iron in basal ganglia. It is a clinically and genetically heterogeneous disorder that is characterized by movement disorders, dystonia, dysarthria, Parkinsonism, intellectual disability, and spasticity. The age at onset varies from childhood to adulthood and the rate of progression is different among affected individuals. Although there is no information about the exact prevalence of NBIA in the world-wide, it is estimated less than 1/1,000,000 in population. NBIAs are inherited in autosomal recessive, autosomal dominant or X-linked fashions. Until now more than 10 genes have been identified for this group of disorders. Among these, only two genes encode proteins that directly involved in iron metabolism. Therefore, how iron contributes to the pathogenesis of NBIA remains unknown. The remaining NBIA-causing genes participate in lipid metabolism, lysosomal functions or autophagy process, and the roles of some of them remain unknown. NBIA is categorized based on the genetic cause of the disease. PKAN, PLAN, MPAN, and BPAN are the most common forms of the disease result from mutations in the PANK2, PLA2G6, C19orf12, and WDR45 genes, respectively. The diagnosis of NBIA is usually based on clinical features and a specific pattern of brain MRI which results from the abnormal accumulation of iron. For example, the pattern of “eye of the tiger” is observed in the brain MRI of PKAN cases. Since, clinical evaluations and neuroimaging have failed in the diagnosis of the disease in some NBIA cases, genetic testing will be helpful. Development of whole-exome sequencing (WES) has facilitated the identification of disease-causing genes but it seems some of NBIA-genes have remained unknown, yet. Identification of novel genes and molecular pathways will enable a deeper understanding of the underlying molecular bases and our knowledge about the pathogenesis of the disease. There is currently no comprehensive study about the NBIA in Iran, however, the latest discovered NBIA gene, GTPBP2, has been identified in an Iranian family.

Published

2020

5. A Pathogenic Homozygous Mutation In The Pleckstrin Homology Domain Of RASA1 Is Responsible For Familial Tricuspid Atresia In An Iranian Consanguineous Family

Author

Ahoura Nozari, Ehsan Aghaei-Moghadam, Aliakbar Zeinaloo, Afagh Alavi, Saghar Ghasemi Firouzabad, Shohre Minaee, Marzeieh Eskandari Hesari, and Farkhondeh Behjati

Subjects

Pleckstrin Homology Domain, RASA1, Tricuspid Atresia, Whole Exome Sequencing, Medicine, Science

Abstract

Objective Tricuspid atresia (TA) is a rare life-threatening form of congenital heart defect (CHD). The genetic mechanisms underlying TA are not clearly understood. According to previous studies, the endocardial cushioning event, as the primary sign of cardiac valvulogenesis, is governed by several overlapping signaling pathways including Ras/ ERK pathway. RASA1, a regulator of cardiovascular development, is involved in this pathway and its haploinsufficiency (due to heterozygous mutations) has been identified as the underlying etiology of the autosomal dominant capillary malformation/arteriovenous malformation (CM/AVM). Materials And Methods In this prospective study, we used whole exome sequencing (WES) followed by serial bioinformatics filtering steps for two siblings with TA and early onset CM. Their parents were consanguineous which had a history of recurrent abortions. Patients were carefully assessed to exclude extra-cardiac anomalies. Results We identified a homozygous RASA1 germline mutation, c.1583A>G (p.Tyr528Cys) in the family. This mutation lies in the pleckstrin homology (PH) domain of the gene. The parents who were heterozygous for this variant displayed CM. Conclusion This is the first study reporting an adverse phenotypic outcome of a RASA1 homozygous mutation. Here, we propose that the phenotypic consequence of the homozygous RASA1 p.Tyr528Cys mutation is more serious than the heterozygous type. This could be responsible for the TA pathogenesis in our patients. We strongly suggest that parents with CM/AVM should be investigated for RASA1 heterozygous mutations. Prenatal diagnosis and fetal echocardiography should also be carried out in the event of pregnancy in heterozygous parents.

Published

2018

6. Description of combined ARHSP/JALS phenotype in some patients with SPG11 mutations

Author

Marzieh Khani, Hosein Shamshiri, Farzad Fatehi, Mohammad Rohani, Bahram Haghi Ashtiani, Fahimeh Haji Akhoundi, Afagh Alavi, Hamidreza Moazzeni, Hanieh Taheri, Mina Tolou Ghani, Leila Javanparast, Seyyed Saleh Hashemi, Ramona Haji‐Seyed‐Javadi, Matineh Heidari, Shahriar Nafissi, and Elahe Elahi

Subjects

ALS, ARHSP, autosomal recessive hereditary spastic paraplegia, juvenile amyotrophic lateral sclerosis, SPG11, Genetics, QH426-470

Abstract

Abstract Background SPG11 mutations can cause autosomal recessive hereditary spastic paraplegia (ARHSP) and juvenile amyotrophic lateral sclerosis (JALS). Because these diseases share some clinical presentations and both can be caused by SPG11 mutations, it was considered that definitive diagnosis may not be straight forward. Methods The DNAs of referred ARHSP and JALS patients were exome sequenced. Clinical data of patients with SPG11 mutations were gathered by interviews and neurological examinations including electrodiagnosis (EDX) and magnetic resonance imaging (MRI). Results Eight probands with SPG11 mutations were identified. Two mutations are novel. Among seven Iranian probands, six carried the p.Glu1026Argfs*4‐causing mutation. All eight patients had features known to be present in both ARHSP and JALS. Additionally and surprisingly, presence of both thin corpus callosum (TCC) on MRI and motor neuronopathy were also observed in seven patients. These presentations are, respectively, key suggestive features of ARHSP and JALS. Conclusion We suggest that rather than ARHSP or JALS, combined ARHSP/JALS is the appropriate description of seven patients studied. Criteria for ARHSP, JALS, and combined ARHSP/JALS designations among patients with SPG11 mutations are suggested. The importance of performing both EDX and MRI is emphasized. Initial screening for p.Glu1026Argfs*4 may facilitate SPG11 screenings in Iranian patients.

Published

2020

7. A novel nonsense mutation in WNK1/HSN2 associated with sensory neuropathy and limb destruction in four siblings of a large Iranian pedigree

Author

Behrouz Rahmani, Fatemeh Fekrmandi, Keivan Ahadi, Tannaz Ahadi, Afagh Alavi, Abolhassan Ahmadiani, and Sareh Asadi

Subjects

Hereditary sensory and autonomic neuropathies, HSAN2, Nonsense mutation, Whole exome sequencing, WNK1 gene, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Hereditary sensory and autonomic neuropathy type 2 (HSAN2) is an autosomal recessive disorder with predominant sensory dysfunction and severe complications such as limb destruction. There are different subtypes of HSAN2, including HSAN2A, which is caused by mutations in WNK1/HSN2 gene. Methods An Iranian family with four siblings and autosomal recessive inheritance pattern whom initially diagnosed with HSAN2 underwent whole exome sequencing (WES) followed by segregation analysis. Results According to the filtering criteria of the WES data, a novel candidate variation, c.3718C > A in WNK1/HSN2 gene that causes p.Tyr1025* was identified. This variation results in a truncated protein with 1025 amino acids instead of the wild-type product with 2645 amino acids. Sanger sequencing revealed that the mutation segregates with disease status in the pedigree. Conclusions The identified novel nonsense mutation in WNK1/HSN2 in an Iranian HSAN2 pedigree presents allelic heterogeneity of this gene in different populations. The result of current study expands the spectrum of mutations of the HSN2 gene as the genetic background of HSAN2A as well as further supports the hypothesis that HSN2 is a causative gene for HSAN2A. However, it seems that more research is required to determine the exact effects of this product in the nervous system.

Published

2018

8. An Iranian familial amyotrophic lateral sclerosis pedigree with p.Val48Phe causing mutation in SOD1: a genetic and clinical report

Author

Afagh Alavi, Marzieh Khani, Shahriar Nafissi, Hosein Shamshiri, and Elahe Elahi

Subjects

ALS Aamyotrophic lateral sclerosis SOD1 Superoxide dismutase 1 gene p.Val48Phe, Medicine

Abstract

Objective(s): Amyotrophic lateral sclerosis (ALS), a fatal progressive neurodegenerative disorder, is the most common motor neuron disease in European populations. Approximately 10% of ALS cases are familial (FALS) and the other patients are considered as sporadic ALS (SALS). Among many ALS causing genes that have been identified, mutations in SOD1 and C9orf72 are the most common genetic causes of the disease. In Iranian patients, it has been shown that SOD1, as compared to C9orf72, plays a much more prominent role. To date, more than 170 mutations have been reported in SOD1. Genotype/phenotype correlation with respect to either different causative genes or different mutations of a specific gene has not been well established. Materials and Methods: Five exons of SOD1 and flanking intronic sequences of an Iranian FALS proband were screened for mutations by direct sequencing. Also, the clinical features of the proband were described. Results: Heterozygous p.Val48Phe causing mutation was identified in SOD1. Age at onset was 29 years and site of the first presentation was the lower extremity in the proband. Conclusion: The p.Val48Phe causing mutation appears to cause early onset of ALS.

Published

2014

9. NMNAT1 and hereditary spastic paraplegia (HSP): expanding the phenotypic spectrum of NMNAT1 variants

Author

Zahra Sadr, Aida Ghasemi, Mohammad Rohani, and Afagh Alavi

Subjects

Neurology, Pediatrics, Perinatology and Child Health, Neurology (clinical), Genetics (clinical)

Published

2023

10. Description of Phenotypic Heterogeneity in a GJC2-Related Family and Literature Review

Author

Aida Ghasemi, Ali Reza Tavasoli, Mana Khojasteh, Mohammad Rohani, and Afagh Alavi

Subjects

Genetics, Genetics (clinical)

Abstract

Introduction: Homozygous and compound heterozygous variants in GJC2, the gene encoding connexin-47 protein, cause Pelizaeus-Merzbacher-like disease type 1 or hypomyelinating leukodystrophy 2 (HLD2), a severe infantile-onset hypomyelinating leukodystrophy, and rarely some milder phenotypes like hereditary spastic paraplegia (HSP) type 44 (SPG44) and subclinical leukodystrophy. Herein, we report an Iranian GJC2-related family with intrafamilial phenotypic heterogeneity and review the literatures. Methods: Whole-exome sequencing was performed for an Iranian proband, who was initially diagnosed as HSP case. Data were analyzed and the candidate variant was confirmed by PCR and Sanger sequencing subsequently checked in family members to co-segregation analysis. A careful clinical and paraclinical evaluation of all affected individuals of the family was done and compared with previous reported GJC2-related families. Results: A novel homozygous variant, c.G14T:p.Ser5Ile, in the GJC2 gene was identified. The variant was co-segregated with the disease status in the family members. Clinical evaluation of all patients showed two distinct GJC2-related phenotypes in this family; the proband presented a complicated form of HSP, whereas both his affected sisters presented a HLD2 phenotype. Discussion: Up to now, correlation between HSP and GJC2 variants has been reported once. Here, the second case of SPG44 was identified that emphasizes on GJC2 as a HSP-causing gene. So, the screening of GJC2 in patients with HSP or HSP-like phenotypes especially with hypomyelination in their brain MRI is recommended. Also, for the first time, intrafamilial phenotypic heterogeneity for “two distinct GJC2-related phenotypes: HLD2 and HSP” was reported. Such intrafamilial phenotypic heterogeneity for GJC2 can emphasize on the shared pathophysiology of these disorders.

Published

2023

11. Familial Hypermanganesemia in Iran

Author

Seyedeh Narges Tabatabaee, Sajjad Effat Nejad, Ali Nikkhah, Narges Hashemi, Afagh Alavi, Anthony E. Lang, Mohammad Rohani, and Maziar Emamikhah

Subjects

Neurology, Neurology (clinical)

Published

2023

12. A Mild Form of Neurodegeneration with Brain Iron Accumulation attributed to Coenzyme A Synthase Mutation

Author

Narges Hashemi, Reza Nejad Shahrokh Abadi, Afagh Alavi, Ali Reza Tavasoli, and Mohammad Rohani

Subjects

Neurology, Neurology (clinical)

Published

2022

13. A founder mutation in COQ7, p.(Leu111Pro), causes pure hereditary spastic paraplegia (HSP) in the Iranian population

Author

Zahra Sadr, Davood Zare-Abdollahi, Mohammad Rohani, and Afagh Alavi

Subjects

Psychiatry and Mental health, Neurology (clinical), Dermatology, General Medicine

Published

2023

14. Anticipation Can Be More Common in Hereditary Spastic Paraplegia with SPAST Mutations Than It Appears

Author

Atefeh Davarzani, Mohammad Rohani, Hossein Najmabadi, Afagh Alavi, Seyyed-Saleh Hashemi, Mohammad Masoud Rahimi Bidgoli, Fardad DanaeeFard, Shahriar Nafissi, Farzad Fatehi, Ariana Kariminejad, and Reza Hajati

Subjects

Genetics, Proband, Sanger sequencing, Candidate gene, Hereditary spastic paraplegia, General Medicine, Disease, Biology, medicine.disease, symbols.namesake, Neurology, Anticipation (genetics), medicine, symbols, Neurology (clinical), Multiplex ligation-dependent probe amplification, Gene

Abstract

Background and objective:Hereditary spastic paraplegia (HSP) is a heterogeneous neurodegenerative disorder with lower-limb spasticity and weakness. Different patterns of inheritance have been identified in HSP. Most autosomal-dominant HSPs (AD-HSPs) are associated with mutations of the SPAST gene (SPG4), leading to a pure form of HSP with variable age-at-onset (AAO). Anticipation, an earlier onset of disease, as well as aggravation of symptoms in successive generations, may be correlated to SPG4. Herein, we suggested that anticipation might be a relatively common finding in SPG4 families.Methods:Whole-exome sequencing was done on DNA of 14 unrelated Iranian AD-HSP probands. Data were analyzed, and candidate variants were PCR-amplified and sequenced by the Sanger method, subsequently checked in family members to co-segregation analysis. Multiplex ligation-dependent probe amplification (MLPA) was done for seven probands. Clinical features of the probands were recorded, and the probable anticipation was checked in these families. Other previous reported SPG4 families were investigated to anticipation.Results:Our findings showed that SPG4 was the common subtype of HSP; three families carried variants in the KIF5A, ATL1, and MFN2 genes, while five families harbored mutations in the SPAST gene. Clinical features of only SPG4 families indicated decreasing AAO in affected individuals of the successive generations, and this difference was significant (p-value Conclusion:It seems SPAST will be the first candidate gene in families that manifests a pure form of AD-HSP and anticipation. Therefore, it may be a powerful situation of genotype–phenotype correlation. However, the underlying mechanism of anticipation in these families is not clear yet.

Published

2021

15. Neurodegeneration with Brain Iron Accumulation and a Brief Report of the Disease in Iran

Author

Mohammad Rohani, Reza Hajati, Afagh Alavi, Fardad Danaee Fard, and Maziar Emamikhah

Subjects

0301 basic medicine, Neurodegeneration with brain iron accumulation, Iron, Disease, Iran, Bioinformatics, Basal Ganglia, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Dystonia, biology, business.industry, Genetic heterogeneity, Parkinsonism, Brain, Ceruloplasmin, General Medicine, medicine.disease, Iron Metabolism Disorders, Ferritin light chain, 030104 developmental biology, Neurology, Mutation, biology.protein, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

Neurodegeneration with brain iron accumulation (NBIA) is a term used for a group of hereditary neurological disorders with abnormal accumulation of iron in basal ganglia. It is clinically and genetically heterogeneous with symptoms such as dystonia, dysarthria, Parkinsonism, intellectual disability, and spasticity. The age at onset and rate of progression are variable among individuals. Current therapies are exclusively symptomatic and unable to hinder the disease progression. Approximately 16 genes have been identified and affiliated to such condition with different functions such as iron metabolism (only two genes: Ferritin Light Chain (FTL) Ceruloplasmin (CP)), lipid metabolism, lysosomal functions, and autophagy process, but some functions have remained unknown so far. Subgroups of NBIA are categorized based on the mutant genes. Although in the last 10 years, the development of whole-exome sequencing (WES) technology has promoted the identification of disease-causing genes, there seem to be some unknown genes and our knowledge about the molecular aspects and pathogenesis of NBIA is not complete yet. There is currently no comprehensive study about the NBIA in Iran; however, one of the latest discovered NBIA genes, GTP-binding protein 2 (GTPBP2), has been identified in an Iranian family, and there are some patients who have genetically remained unknown.

Published

2021

16. A case of adult onset Sandhoff disease that mimics Brown-Vialetto-Van Laere syndrome

Author

Elahe Elahi, Shahriar Nafissi, Niloofar Farboodi, Hanieh Taheri, Hamid Ahmadieh, Hamidreza Moazzeni, Hosein Shamshiri, Marzieh Khani, and Afagh Alavi

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, business.industry, Sandhoff disease, Compound heterozygosity, medicine.disease, HEXB, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Neurology, Brown–Vialetto–Van Laere syndrome, Pediatrics, Perinatology and Child Health, Medicine, Cerebellar atrophy, Neurology (clinical), Differential diagnosis, business, 030217 neurology & neurosurgery, Genetics (clinical), Exome sequencing, Hexosaminidase activity

Abstract

Sandhoff disease is a rare fatal infantile neurologic disorder. Adult onset Sandhoff is even rarer. Variability of clinical features in adult onset Sandhoff patients and overlaps between these and features of other neurologic diseases have sometimes led to mis-diagnosis. We describe an adult onset Sandhoff disease affected individual whose clinical presentation were also consistent with the Brown-Vialetto-Van Laere syndrome (BVVL) diagnosis. Screening of BVVL-causing genes, SLC52A3 and SLC52A2, did not identify candidate disease-causing mutations, but exome sequencing revealed compound heterozygous mutations in the known Sandhoff disease-causing gene, HEXB. Decreased blood hexosaminidase activity and evidence of cerebellar atrophy confirmed Sandhoff disease diagnosis. To the best of our knowledge, this is the first report of a Sandhoff disease case that mimics BVVL and that presents with prominent cranial nerve involvement. For differential diagnosis, measurement of hexosaminidase activity and MRI should quickly be performed. Genetic analysis can be done for confirmation of diagnosis.

Published

2021

17. Clinical spectrum in multiple families with primary <scp> COQ 10 </scp> deficiency

Author

Seyyed Saleh Hashemi, Mohammad Kazem Bakhshandeh, Davood Zare-Abdollahi, Fardad DanaeeFard, Kolsoum Inanloo Rahatloo, Niloofar Farboodi, Afagh Alavi, Amirreza Vafaee, Sona Abolhasani, and Mohammad Rohani

Subjects

Coenzyme Q10, Genetics, Heterogeneous group, Hereditary spastic paraplegia, Mitochondrial disease, Biology, medicine.disease, chemistry.chemical_compound, chemistry, medicine, COQ7, Atp production, Coenzyme Q10 deficiency, Gene, Genetics (clinical)

Abstract

Coenzyme Q10/ COQ10 , an essential cofactor in the electron-transport chain is involved in ATP production. Primary COQ10 deficiency is clinically and genetically a heterogeneous group of mitochondrial disorders caused by defects in the COQ10 synthesis pathway. Its mode of inheritance is autosomal recessive and it is characterized by metabolic abnormalities and multisystem involvement including neurological features. Mutations in 10 genes have been identified concerning this group of diseases, so far. Among those, variants of the COQ7 gene are very rare and confined to three patients with Asian ancestry. Here, we present the clinical features and results of whole-exome sequencing (WES) of three Iranian unrelated families affected by primary COQ10 deficiency. Three homozygous variants in COQ2, COQ4, and COQ7 genes were identified. Candidate variants of the COQ2 and COQ4 genes were novel and associated with the cerebellar signs and multisystem involvement, whereas, the known variant in COQ7 was associated with a mild phenotype that was initially diagnosed as hereditary spastic paraplegia (HSP). This variant has already been reported in a Canadian girl with similar presentations that also originated from Iran suggesting both patients may share a common ancestor. Due to extensive heterogeneity in this group of disorders, and overlap with other mitochondrial/neurological disorders, WES may be helpful to distinguish primary coenzyme Q10 deficiency from other similar conditions. Given that some features of primary coenzyme Q10 deficiency may improve with exogenous COQ10 , early diagnosis is very important.

Published

2020

18. Putative founder effect in the Polish, Iranian and United States populations for the L144S SOD1 mutation associated with slowly uniform phenotype of amyotrophic lateral sclerosis

Author

Elahe Elahi, Cezary Żekanowski, Afagh Alavi, Peter M. Andersen, Mariusz Berdynski, Peter C. Sapp, Mitsuya Morita, and Magdalena Kuźma-Kozakiewicz

Subjects

Genetics, medicine.medical_specialty, Neurology, SOD1, Str markers, Biology, medicine.disease, Phenotype, 03 medical and health sciences, 0302 clinical medicine, Mutation (genetic algorithm), medicine, Neurology (clinical), Amyotrophic lateral sclerosis, 030217 neurology & neurosurgery, Founder effect

Abstract

Mutations inSOD1cause approximately 12-25% of familial ALS and approximate to 2% of apparently sporadic ALS cases. Clinical phenotypes linked to SOD1 mutations are heterogeneous and intra-familial ...

Published

2020

19. CAPN1 and hereditary spastic paraplegia: a novel variant in an Iranian family and overview of the genotype-phenotype correlation

Author

Mohammad Rohani, Afagh Alavi, Hossein Najmabadi, Babak Zamani, Mohammad Masoud Rahimi Bidgoli, and Leila Javanparast

Subjects

0301 basic medicine, Genetics, CAPN1 Gene, Hereditary spastic paraplegia, General Neuroscience, General Medicine, Biology, musculoskeletal system, medicine.disease, nervous system diseases, Genotype phenotype, 03 medical and health sciences, Inheritance (object-oriented programming), 030104 developmental biology, 0302 clinical medicine, medicine, 030217 neurology & neurosurgery

Abstract

SPG76 is one of the rare forms of hereditary spastic paraplegia (HSP) which causes by mutations in the CAPN1 gene. The mode of inheritance of SPG76 is autosomal recessive (AR) and so far, only 24 f...

Published

2020

20. Mutation in ALOX12B likely cause of POI and also ichthyosis in a large Iranian pedigree

Author

Mohammad Masoud Rahimi Bidgoli, Judith Fischer, Faezeh Darki, Mostafa Mirshams Shahshahani, Elahe Elahi, Ashraf Moini, Afagh Alavi, and Davood Zare-Abdollahi

Subjects

Adult, 0106 biological sciences, 0301 basic medicine, Genetic Linkage, Anion Transport Proteins, Menopause, Premature, ALOX12B, Locus (genetics), Iran, Primary Ovarian Insufficiency, Biology, Arachidonate 12-Lipoxygenase, Premature ovarian insufficiency, 01 natural sciences, Consanguinity, 03 medical and health sciences, Genetic linkage, Exome Sequencing, Genetics, medicine, Humans, Genetic Predisposition to Disease, Molecular Biology, Exome sequencing, Ichthyosis, Homozygote, General Medicine, Lipid Metabolism, Disease gene identification, medicine.disease, Human genetics, Pedigree, 030104 developmental biology, Mutation, Female, 010606 plant biology & botany

Abstract

Premature ovarian insufficiency (POI) is a clinically and etiologically heterogeneous disorder characterized by menstrual irregularities and elevated levels of FSH before age of 40 years. Genetic anomalies are among the recognized causes of POI. Here, we aimed to identify the genetic cause of POI in an inbred pedigree with nine POI and two ichthyosis-affected members. Inheritance of POI and ichthyosis were, respectively, dominant and recessive. Reproduction-related information and measurements of relevant hormones were obtained. Genetic studies included homozygosity mapping, linkage analysis, exome sequencing, and screening of candidate variants. A mutation within ALOX12B, which is a known ichthyosis causing gene, was identified as cause of ichthyosis. ALOX12B encodes a protein involved in steroidogenesis and lipid metabolism. Considering the importance of steroidogenesis in reproduction functions, the possibility that the ALOX12B mutation is also cause of POI was considered. Screenings showed that the mutation segregated with POI status. Linkage analysis with respect to POI identified a single strongly linked locus (LOD > 3) that includes ALOX12B. Exome sequencing on POI-affected females identified the mutation in ALOX12B and also a sequence variation in SPNS2 within the linked locus. A possible contribution of the SPNS2 variation to POI was not strictly ruled out, but various data presented in the text including reported association of variations in related gene ALOX12 with menopause-age and role of ALOX12B in atretic bovine follicle formation argue in favor of ALOX12B. It is, therefore, concluded that the mutation in ALOX12B is the likely cause of POI in the pedigree.

Published

2020

21. Giant axonal neuropathy: The first Iranian case with a variation in the gigaxonin gene and a glance to the other cases

Author

Masood Ghahvechi-Akbar, Reza Hajati, Davood Zare-Abdollahi, Afagh Alavi, Saeideh Ghasemi, Leila Tahernia, Mohammad Vafaee-Shahi, and Atefeh Davarzani

Subjects

Proband, Sanger sequencing, Pathology, medicine.medical_specialty, Ataxia, business.industry, Genetic counseling, Short Communication, Gigaxonin, medicine.disease, Whole Exome Sequencing, symbols.namesake, Neurology, Giant Axonal Neuropathy, symbols, Medicine, GAN Protein, Allelic heterogeneity, Neurology (clinical), medicine.symptom, business, Menkes Kinky Hair Syndrome, Exome sequencing, Giant axonal neuropathy

Abstract

Background: Giant axonal neuropathy (GAN) is a very rare fatal neurodegenerative disorder with clinical and allelic heterogeneity. The disease is caused by mutations in the GAN (gigaxonin) gene. Herein, we reported the clinical presentations and results of genetic analysis of the first Iranian GAN case. Methods: Phenotypic data were obtained by neurologic examination, brain magnetic resonance imaging (MRI), electromyography (EMG), electroencephalography (EEG), and sonography from the proband. Deoxyribonucleic acid (DNA) was isolated from peripheral blood leucocytes and whole exome sequencing (WES) was performed. The candidate variant was screened by Sanger sequencing in the proband and her family members. Results: The proband was a 7-year-old girl who was admitted with a chief complaint of ataxia, muscle weakness, delayed developmental milestones, and history of psychiatric disorders. She was very moody and had clumsy gait, decreased deep tendon reflexes (DTRs) of lower limbs, and kinky hair. The brain MRI revealed white matter abnormality. The EMG revealed that her disease was compatible with the chronic axonal type of sensorimotor polyneuropathy; however, her EEG was normal. Results of the WES revealed a homozygous variant; c.G778T:p.E260* in the GAN gene, indicating the GAN disorder. Conclusion: The present study affirmed GAN allelic heterogeneity and resulted in the expansion of the phenotypic spectrum of GAN pathogenic variants. Identification of more families with mutations in GAN gene helps to further understand the molecular basis of the disease and provides an opportunity for genetic counseling especially in the populations with a high degree of consanguineous marriage such as the Iranian population.

Published

2020

22. Intellectual disability associated with craniofacial dysmorphism due to POLR3B mutation and defect in spliceosomal machinery

Author

Mostafa Saghi, Kolsoum InanlooRahatloo, Afagh Alavi, Kimia Kahrizi, and Hossein Najmabadi

Subjects

Ribosomal Proteins, Intellectual Disability, Mutation, Genetics, Mutation, Missense, Spliceosomes, Humans, RNA Polymerase III, Genetics (clinical), Pedigree, Transcription Factors

Abstract

Background Intellectual disability (ID) is a clinically important disease and a most prevalent neurodevelopmental disorder. The etiology and pathogenesis of ID are poorly recognized. Exome sequencing revealed a homozygous missense mutation in the POLR3B gene in a consanguineous family with three Intellectual disability with craniofacial anomalies patients. POLR3B gene encoding the second largest subunit of RNA polymerase III. Methods We performed RNA sequencing on blood samples to obtain insights into the biological pathways influenced by POLR3B mutation. We applied the results of our RNA-Seq analysis to several gene ontology programs such as ToppGene, Enrichr, KEGG. Results A significant decrease in expression of several spliceosomal RNAs, ribosomal proteins, and transcription factors was detected in the affected, compared to unaffected, family members. Conclusions We hypothesize that POLR3B mutation dysregulates the expression of some important transcription factors, ribosomal and spliceosomal genes, and impairments in protein synthesis and splicing mediated in part by transcription factors such as FOXC2 and GATA1 contribute to impaired neuronal function and concurrence of intellectual disability and craniofacial anomalies in our patients. Our study highlights the emerging role of the spliceosome and ribosomal proteins in intellectual disability.

Published

2021

23. Anticipation Can Be More Common in Hereditary Spastic Paraplegia with

Author

Seyyed-Saleh, Hashemi, Reza, Hajati, Atefeh, Davarzani, Mohammad, Rohani, Fardad, DanaeeFard, Mohammad Masoud, Rahimi Bidgoli, Farzad, Fatehi, Ariana, Kariminejad, Hossein, Najmabadi, Shahriar, Nafissi, and Afagh, Alavi

Subjects

Adenosine Triphosphatases, Phenotype, Spastin, GTP-Binding Proteins, Spastic Paraplegia, Hereditary, Mutation, Humans, Kinesins, Membrane Proteins, Iran

Abstract

Hereditary spastic paraplegia (HSP) is a heterogeneous neurodegenerative disorder with lower-limb spasticity and weakness. Different patterns of inheritance have been identified in HSP. Most autosomal-dominant HSPs (AD-HSPs) are associated with mutations of theWhole-exome sequencing was done on DNA of 14 unrelated Iranian AD-HSP probands. Data were analyzed, and candidate variants were PCR-amplified and sequenced by the Sanger method, subsequently checked in family members to co-segregation analysis. Multiplex ligation-dependent probe amplification (MLPA) was done for seven probands. Clinical features of the probands were recorded, and the probable anticipation was checked in these families. Other previous reported SPG4 families were investigated to anticipation.Our findings showed that SPG4 was the common subtype of HSP; three families carried variants in theIt seems

Published

2021

24. The second family affected with a PRDM8-related disease

Author

Atefeh Davarzani, Amin Shahrokhi, Seyyed Saleh Hashemi, Aida Ghasemi, Mohammad Reza Habibi Kavashkohei, Niloofar Farboodi, Anthony E. Lang, Maryam Ghiasi, Mohammad Rohani, and Afagh Alavi

Subjects

Spastic Paraplegia, Hereditary, Ubiquitin-Protein Ligases, Dermatology, General Medicine, Iran, Myoclonic Epilepsies, Progressive, DNA-Binding Proteins, Psychiatry and Mental health, Lafora Disease, Seizures, Mutation, Histone Methyltransferases, Humans, Neurology (clinical), Carrier Proteins

Abstract

Lafora disease (LD) is a severe form of progressive myoclonus epilepsy characterized by generalized seizures, myoclonus, intellectual decline, ataxia, spasticity, dysarthria, visual loss, and in later stages, psychosis and dementia. To date, mutations in the EPM2A and EPM2B/NHLRC1 genes have been identified as the common causes of LD. However, a mutation in PRDM8 has been reported only once in a Pakistani family affected with early-onset Lafora disease. In the present study, we report the second family with a PRDM8 mutation.Two affected individuals of an Iranian family initially diagnosed as complicated hereditary spastic paraplegia (HSP) underwent careful neurologic examination. Homozygosity mapping and whole-exome sequencing were performed. Based on the results of genetic analysis to detection of Lafora bodies, a skin biopsy was done.The clinical features of the patients were described. Linkage to chromosome 4 and a mutation in the PRDM8 gene were identified, suggesting the patients may be affected with early-onset LD. However, like the Pakistani family, the search for Lafora bodies in their skin biopsies was negative. Their electroencephalograms showed generalized epileptiform discharges in the absence of clinical seizures.The current study increases the number of PRDM8-related cases and expands the phenotypic spectrum of mutations in the PRDM8 gene. Both reported PRDM8-related families presented intra and inter-familial heterogeneity and they have originated from the Middle East. Thus, it seems the PRDM8 mutations should be considered not only in LD but also in other neurodegenerative disorders such as a complicated HSP-like phenotype, especially in this region.

Published

2021

25. Study on SARS-CoV-2 strains in Iran reveals potential contribution of co-infection with and recombination between different strains to the emergence of new strains

Author

Amir Masoud Hashemian, Saeid Amel Jamehdar, Hadi Razavi Nikoo, Issa Jahanzad, Mehdi Sepehrnejad, Abtin Heidarzadeh, Peyman Taghizadeh, Mohammad Masoud Rahimi Bidgoli, Arash Shakibzadeh, Hamid Galehdari, Hadi Yari, Mohammad Reza Haghshenas, Sadegh Salehi, Seyed Massoud Houshmand, Iman Safari, Noorossadat Seyyedi, Elham Kheyrani, Nayebali Rezvani, Gholamreza Shariati, Elahe Elahi, Forouzandeh Mahjoubi, Mohammad Hossein Sanati, Afagh Alavi, Ahmad Piroozmand, Ali Mojtahedi, Seyed Mohammadsaleh Zahraei, Ali Heshmati, Kolsoum InanlooRahatloo, and Soroosh Dabiri

Subjects

Genotyping Techniques, Genome, Viral, Biology, Iran, Genome, Article, law.invention, Evolution, Molecular, 03 medical and health sciences, Recombinant genomes, law, Virology, Humans, Clade, Genotyping, Phylogeny, 030304 developmental biology, Genetics, Recombination, Genetic, 0303 health sciences, Coinfection, SARS-CoV-2, Tag nucleotide genotyping, 030302 biochemistry & molecular biology, Haplotype, RNA, COVID-19, Genetic Variation, Amplicon, Co-infection, Haplotypes, Mutation, Recombinant DNA, RNA, Viral, Recombination

Abstract

We aimed to describe SARS-CoV-2 strains in Iranians from nine distributed cities infected during two months expanding late 2020 and early 2021 by genotyping known informative single nucleotide in five PCR amplicons. Two variants associated with haplotype H1 (clade G) and nine additional variants associated with other haplotypes were genotyped, respectively, in RNA isolates of 244 and 85 individuals. The variants associated with the H1a (GR) and H1b (GH) haplotypes were most prevalent, indicating a significant change in infection pattern with passage of time. The most important findings were that recombinant genomes and co-infection, respectively, were surmised in 44.7% and 12.9% of the samples extensively genotyped. Partners of many of the recombinations were relatively common strains. Co-existing viruses were among those currently circulating in Iran. In addition to random mutations, co-infection with different existing strains and recombination between their genomes may significantly contribute to the emergence of new SARS-CoV-2 strains.

Published

2021

26. MFSD8 gene mutations; evidence for phenotypic heterogeneity

Author

Mohammad Dehani, Hamid Reza Khorram Khorshid, Alireza Dehghani, Ata Bushehri, Davood Zare-Abdollahi, Seyed Ali Mohammad Miratashi, Jalil Effati, Afagh Alavi, Payman Jamali, and Mohammadreza Mousavi-Mirkala

Subjects

Adult, Male, 0301 basic medicine, genetic structures, Genetic counseling, Mutation, Missense, Vision Disorders, Visual Acuity, Iran, 030105 genetics & heredity, Gene mutation, Biology, Compound heterozygosity, Consanguinity, Genetic Heterogeneity, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, Neuronal Ceroid-Lipofuscinoses, Exome Sequencing, Humans, Fluorescein Angiography, Allele, Genetics (clinical), Genetics, Sanger sequencing, Genetic heterogeneity, Membrane Transport Proteins, Dystrophy, Macular dystrophy, Pedigree, Ophthalmology, Phenotype, Pediatrics, Perinatology and Child Health, 030221 ophthalmology & optometry, symbols, Female, sense organs, Visual Fields, Cone-Rod Dystrophies, Tomography, Optical Coherence

Abstract

BACKGROUND Cone-rod dystrophies are a group of genetically and phenotypically heterogeneous inherited degenerative retinal diseases primarily affecting macular and cone system function. MFSD8 loss-of-function variants are mainly related to the variant late-infantile neuronal ceroid lipofuscinoses which present with progressive motor and mental regression in combination with seizures, ataxia, and visual impairment. MATERIAL AND METHODS Clinical examination and genomic DNA extraction were collected from two unrelated Iranian families presenting with autosomal recessive cone-rod dystrophy. The candidate disease-causing variant was screened with whole-exome sequencing and bioinformatics analyses. Sanger sequencing was used for validation and co-segregation analysis. RESULTS Two previously reported variants (c.1361T>C; p.M454T and c.1235C>T; p.P412L) and in a compound heterozygous pattern in one family and a homozygous variant (c.1361T>C; p.M454T) identical to one of the variants in the first family in MFSD8 gene were identified. Both confirmed by Sanger sequencing and co-segregated with disease status. CONCLUSIONS Here and for the first time, we reported on two previously variant late-infantile neuronal ceroid lipofuscinoses-associated variants in MFSD8 but in association with a form of cone-rod dystrophy known as non-syndromic macular dystrophy with central cone involvement. Our results support this concept that variant late-infantile neuronal ceroid lipofuscinoses and non-syndromic macular dystrophy with central cone involvement are not different disease entities, but rather allelic diseases and phenotypic variants of the same mutation. Consideration of the milder MFSD8 phenotypes is important against the potentially severe consequences of life-threatening conditions associated with MFSD8 mutations in order to prevent the danger of misdiagnosis as well as the accuracy of genetic counseling.

Published

2019

27. Spinocerebellar Ataxia 40: Another Etiology Underlying Essential Tremor Syndrome

Author

Fatemeh Moghadas, Renato P. Munhoz, Maziar Emamikhah, Afagh Alavi, Anthony E. Lang, Sharmin Aghavali, and Mohammad Rohani

Subjects

Ataxia, Neurology, Essential tremor, business.industry, Etiology, Spinocerebellar ataxia, Medicine, Neurology (clinical), Case Reports, medicine.symptom, business, medicine.disease, Neuroscience

Published

2021

28. Description of clinical features and genetic analysis of one ultra-rare (SPG64) and two common forms (SPG5A and SPG15) of hereditary spastic paraplegia families

Author

Reza Hajati, Atefeh Davarzani, Mahdieh Pashaei, Farzaneh Larti, Afagh Alavi, Babak Zamani, Shahriar Nafissi, Mohammad Rohani, and Yalda Nilipour

Subjects

0301 basic medicine, Proband, Adult, Male, Adolescent, Hereditary spastic paraplegia, Cytochrome P450 Family 7, Disease, Biology, Genetic analysis, 03 medical and health sciences, Cellular and Molecular Neuroscience, Young Adult, 0302 clinical medicine, Exome Sequencing, Genetics, medicine, Humans, Child, Gene, Genetic heterogeneity, Spastic Paraplegia, Hereditary, Apyrase, medicine.disease, Phenotype, Pedigree, 030104 developmental biology, Child, Preschool, Mutation, Steroid Hydroxylases, Allelic heterogeneity, Female, Carrier Proteins, 030217 neurology & neurosurgery

Abstract

Hereditary spastic paraplegia (HSP) is a clinically and genetically heterogeneous neurodegenerative disorder, characterized by lower-limb spasticity and weakness. To date, more than 82 loci/genes (SPG1-SPG82) have been identified that contribute to the cause of HSP. Despite the use of next-generation sequencing-based methods, genetic-analysis has failed in the finding of causative genes in more than 50% of HSP patients, indicating a more significant heterogeneity and absence of a given phenotype-genotype correlation. Here, we performed whole-exome sequencing (WES) to identify HSP-causing genes in three unrelated-Iranian probands. Candidate variants were detected and confirmed in the probands and co-segregated in the family members. The phenotypic data gathered and compared with earlier cases with the same sub-types of disease. Three novel homozygous variants, c.978delT; p.Q327Kfs*39, c.A1208G; p.D403G and c.3811delT; p.S1271Lfs*44, in known HSP-causing genes including ENTPD1, CYP7B1, and ZFYVE26 were identified, respectively. Intra and interfamilial clinical variability were observed among affected individuals. Mutations in CYP7B1 and ZFYVE26 are relatively common causes of HSP and associated with SPG5A and SPG15, respectively. However, mutations in ENTPD1 are related to SPG64 which is an ultra-rare form of HSP. The research affirmed more complexities of phenotypic manifestations and allelic heterogeneity in HSP. Due to these complexities, it is not feasible to show a clear phenotype-genotype correlation in HSP cases. Identification of more families with mutations in HSP-causing genes may help the establishment of this correlation, further understanding of the molecular basis of the disease, and would provide an opportunity for genetic-counseling in these families.

Published

2021

29. LGMD

Author

Lidia Gonzalez-Quereda, Claudio Bruno, E. Dourado, Juan J. Vílchez, Chiara Panicucci, M. Guglierir, N. Kadem, Jorge Alonso-Pérez, Nuria Muelas, Afagh Alavi, M. Umair, Chiara Marini-Bettolo, Edmar Zanoteli, V. Straub, and J. Diaz-Manera

Subjects

Pathology, medicine.medical_specialty, Neurology, business.industry, Pediatrics, Perinatology and Child Health, medicine, Neurology (clinical), Muscular dystrophy, medicine.disease, business, Genetics (clinical), Delta-Sarcoglycan, Large cohort

Published

2021

30. Circulating miRNA biomarkers for sporadic Amyotrophic Lateral Sclerosis: a systematic meta-analysis and empirical validation

Author

Afagh Alavi, Mehdi Mehdizadeh, Mahammad Taghi Joghataei, Babak Zamani, Shahram Teimourian, Mahmood Barati, and Narges Daneshafrooz

Subjects

Circulating mirnas, Oncology, medicine.medical_specialty, business.industry, Internal medicine, Meta-analysis, medicine, Amyotrophic lateral sclerosis, medicine.disease, business

Abstract

Amyotrophic lateral sclerosis (ALS) is a lethal neurodegenerative disease that occurs as sporadic (sALS) in most cases. The disease is not curable, and its pathogenesis is not understood as yet. Given the intricacy of underlying molecular interactions and heterogeneity of ALS, the discovery of molecules contributing to disease onset and progression will open the way for advancement in prevention and therapeutic intervention. Here we conducted a meta-analysis of 12 circulating miRNA profiling studies using the robust rank aggregation (RRA) method, followed by enrichment analysis. We identified miR-451a and let-7f-5p as meta-signature miRNAs whose targets are involved in critical pathogenic pathways underlying ALS, including FoxO, MAPK, and apoptosis. A systematic review of 7 gene profiling studies elucidated that 241 genes upregulated in sALS circulation with concomitant being targets of the meta-signature miRNAs. Protein-protein interaction network analysis for selected targets revealed the main subcluster is involved in multiple cascades, which eventually leads to apoptosis. Besides, evaluation of relative expression of miRNAs by TaqMan RT-qPCR verified let-7f-5p is significantly downregulated in the plasma of patients. Furthermore, we verified the relative expression of two top-ranked upregulated miRNAs and found miR-338-3p significantly upregulated in ALS patients. Receiver operating characteristic (ROC) analysis indicated that let-7f-5p and miR-338-3p are useful plasms biomarkers for diagnosis and a potential therapeutic target for ALS disease.

Published

2021

31. Clinical and genetic spectrum of a large cohort of patients with δ-sarcoglycan muscular dystrophy

Author

Afagh Alavi, Yalda Nilipour, Luca Bello, Jorge Alonso-Pérez, Shahriar Nafissi, Muhammad Umair, Lidia Gonzalez-Quereda, Mario Emilio Dourado, Chiara Marini-Bettolo, Chiara Panicucci, Xavier Suárez-Calvet, Gultekin Kutluk, Kinga Hadzsiev, Lucas Michielon de Augusto Isihi, Edmar Zanoteli, Jordi Díaz-Manera, Thomas O. Crawford, Muhammad Younus, Ana Töpf, Naz Kadem, Elena Pegorano, Juan José Vilchez, Claudio Bruno, Pia Gallano, Béla Melegh, Michela Guglieri, Nuria Muelas, and Volker Straub

Subjects

Adult, medicine.medical_specialty, Weakness, Proximal muscle weakness, Muscular dystrophies, Generalized muscle weakness, SGCD, Muscular Dystrophies, SGCG, Sarcoglycans, Internal medicine, Sarcoglycanopathies, medicine, Humans, Registries, Muscular dystrophy, Child, Retrospective Studies, LGMD-R6/2F, Muscle Weakness, Muscle biopsy, medicine.diagnostic_test, business.industry, Delta-sarcoglycan, Retrospective cohort study, medicine.disease, Muscular Dystrophies, Limb-Girdle, Neurology (clinical), medicine.symptom, business

Abstract

Sarcoglycanopathies include four subtypes of autosomal recessive limb-girdle muscular dystrophies (LGMDR3, LGMDR4, LGMDR5 and LGMDR6) that are caused, respectively, by mutations in the SGCA, SGCB, SGCG and SGCD genes. Delta-sarcoglycanopathy (LGMDR6) is the least frequent and is considered an ultra-rare disease. Our aim was to characterize the clinical and genetic spectrum of a large international cohort of LGMDR6 patients and to investigate whether or not genetic or protein expression data could predict a disease's severity. This is a retrospective study collecting demographic, genetic, clinical and histological data of patients with genetically confirmed LGMDR6 including protein expression data from muscle biopsies. We contacted 128 paediatric and adult neuromuscular units around the world that reviewed genetic data of patients with a clinical diagnosis of a neuromuscular disorder. We identified 30 patients with a confirmed diagnosis of LGMDR6 of which 23 patients were included in this study. Eighty-seven per cent of the patients had consanguineous parents. Ninety-one per cent of the patients were symptomatic at the time of the analysis. Proximal muscle weakness of the upper and lower limbs was the most common presenting symptom. Distal muscle weakness was observed early over the course of the disease in 56.5% of the patients. Cardiac involvement was reported in five patients (21.7%) and four patients (17.4%) required non-invasive ventilation. Sixty per cent of patients were wheelchair-bound since early teens (median age of 12.0 years). Patients with absent expression of the sarcoglycan complex on muscle biopsy had a significant earlier onset of symptoms and an earlier age of loss of ambulation compared to patients with residual protein expression. This study confirmed that delta-sarcoglycanopathy is an ultra-rare neuromuscular condition and described the clinical and molecular characteristics of the largest yet-reported collected cohort of patients. Our results showed that this is a very severe and quickly progressive disease characterized by generalized muscle weakness affecting predominantly proximal and distal muscles of the limbs. Similar to other forms of sarcoglycanopathies, the severity and rate of progressive weakness correlates inversely with the abundance of protein on muscle biopsy. Alonso-Pérez et al. describe the largest cohort to date of patients with the ultra-rare neuromuscular disorder delta-sarcoglycanopathy, and show that the severity and rate of progressive weakness correlates inversely with the abundance of protein expression on muscle biopsy.

Published

2021

32. Congenital Ichthyosis in a Case of Spinocerebellar Ataxia Type 34: A Novel Presentation for a Known Mutation

Author

Fahimeh Hajiakhoundi, Renato P. Munhoz, Ghazal Haeri, Mohammad Rohani, Afagh Alavi, and Maryam Ghiasi

Subjects

medicine.medical_specialty, Ichthyosis, business.industry, medicine.disease, Dermatology, Letters: Genotype and Phenotype, Neurology, Congenital ichthyosis, Mutation (genetic algorithm), medicine, Spinocerebellar ataxia, Neurology (clinical), Presentation (obstetrics), medicine.symptom, business, Hot cross bun sign, Myoclonus

Published

2020

33. BVVL/ FL: features caused by SLC52A3 mutations; WDFY4 and TNFSF13B may be novel causative genes

Author

Peyman Taghizadeh, Hosein Shamshiri, Shaghayegh Eshghi, Shahriar Nafissi, Hanieh Taheri, Ali Heshmati, Susana Carmona, Siamak Abdi, Marzieh Khani, John Hardy, Majid Shahabi, Hamidreza Moazzeni, Yalda Nilipour, Tooba Ghazanfari, Afagh Alavi, Reza Boostani, Giorgio Valle, Mohammad Rohani, Ali Asghar Okhovat, Jose Tomas Bras, and Elahe Elahi

Subjects

0301 basic medicine, Proband, Male, Aging, Bulbar Palsy, Progressive, Biology, Immunologic Tests, medicine.disease_cause, Genetic analysis, 03 medical and health sciences, 0302 clinical medicine, Audiometry, Genotype, B-Cell Activating Factor, medicine, Humans, Genetic Testing, Allele, Amyotrophic lateral sclerosis, Gene, Genetic Association Studies, Genetics, Neurologic Examination, Mutation, General Neuroscience, Muscles, Amyotrophic Lateral Sclerosis, Intracellular Signaling Peptides and Proteins, Membrane Transport Proteins, medicine.disease, Penetrance, Magnetic Resonance Imaging, 030104 developmental biology, Female, Neurology (clinical), Geriatrics and Gerontology, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Brown-Vialetto-Van Laere (BVVL) and Fazio-Londe are disorders with amyotrophic lateral sclerosis-like features, usually with recessive inheritance. We aimed to identify causative mutations in 10 probands. Neurological examinations, genetic analysis, audiometry, magnetic resonance imaging, biochemical and immunological testings, and/or muscle histopathology were performed. Mutations in known causative gene SLC52A3 were found in 7 probands. More importantly, only 1 mutated allele was observed in several patients, and variable expressivity and incomplete penetrance were clearly noted. Environmental insults may contribute to variable presentations. Putative causative mutations in other genes were identified in 3 probands. Two of the genes, WDFY4 and TNFSF13B, have immune-related functions. Inflammatory responses were implicated in the patient with the WDFY4 mutation. Malfunction of the immune system and mitochondrial anomalies were shown in the patient with the TNFSF13B mutation. Prevalence of heterozygous SLC52A3 BVVL causative mutations and notable variability in expressivity of homozygous and heterozygous genotypes are being reported for the first time. Identification of WDFY4 and TNFSF13B as candidate causative genes supports conjectures on involvement of the immune system in BVVL and amyotrophic lateral sclerosis.

Published

2020

34. Clinical spectrum in multiple families with primary COQ

Author

Seyyed S, Hashemi, Davood, Zare-Abdollahi, Mohammad K, Bakhshandeh, Amirreza, Vafaee, Sona, Abolhasani, Kolsoum, Inanloo Rahatloo, Fardad, DanaeeFard, Niloofar, Farboodi, Mohammad, Rohani, and Afagh, Alavi

Subjects

Male, Canada, Alkyl and Aryl Transferases, Mitochondrial Diseases, Muscle Weakness, Ubiquinone, Infant, Newborn, Iran, Mitochondria, Mixed Function Oxygenases, Mitochondrial Proteins, Mutation, Exome Sequencing, Humans, Ataxia, Female, Genetic Predisposition to Disease, Child

Abstract

Coenzyme Q

Published

2020

35. A mutation in

Author

Ensieh, Darbari, Davood, Zare-Abdollahi, Afagh, Alavi, Mozhgan, Rezaei Kanavi, Sepehr, Feizi, Seyed Bagher, Hosseini, Alireza, Baradaran-Rafii, Hamid, Ahmadieh, Shohreh, Issazadeh-Navikas, and Elahe, Elahi

Subjects

Adult, Male, Base Sequence, Vesicular Transport Proteins, Genes, Recessive, Embryo, Mammalian, Pedigree, Consanguinity, Young Adult, Corneal Opacity, Gene Expression Regulation, Anterior Eye Segment, Mutation, Humans, Family, Female, Genetic Predisposition to Disease, Eye Abnormalities, Child

Abstract

Peters anomaly (PA) is a heterogeneous developmental disorder characterized by central corneal opacity and iridocorneal or corneolenticular adhesions. Although many causative genes have been identified, most screened patients do not have mutations in the known genes. We aimed to identify the genetic cause of Peters anomaly in a pedigree with three affected individuals.Slit-lamp biomicroscopy and ultrasound biomicroscopy were performed for definitive diagnosis. Exome sequencing was conducted on the DNA of all three patients. After identification of a candidate causative gene, expression of the gene was assessed with real-time PCR in various ocular tissues of three human embryos and three adults.The patients were affected with isolated PA. The parents of the patients were related to one another. Inheritance of PA was autosomal recessive. After appropriate filtering of the exome data, a homozygous variation in

Published

2020

36. Description of combined ARHSP/JALS phenotype in some patients with SPG11 mutations

Author

Hamidreza Moazzeni, Hanieh Taheri, Seyyed Saleh Hashemi, Farzad Fatehi, Shahriar Nafissi, Mina Tolou Ghani, Elahe Elahi, Afagh Alavi, Fahimeh Haji Akhoundi, Leila Javanparast, Hosein Shamshiri, Ramona Haji-Seyed-Javadi, Marzieh Khani, Matineh Heidari, Mohammad Rohani, and Bahram Haghi Ashtiani

Subjects

0301 basic medicine, Proband, Adult, Male, Pathology, medicine.medical_specialty, lcsh:QH426-470, Electrodiagnosis, ARHSP, Adolescent, Juvenile amyotrophic lateral sclerosis, 030105 genetics & heredity, medicine.disease_cause, Corpus Callosum, Diagnosis, Differential, 03 medical and health sciences, juvenile amyotrophic lateral sclerosis, Genetics, medicine, Humans, Genetic Testing, Molecular Biology, Exome, Genetics (clinical), Mutation, autosomal recessive hereditary spastic paraplegia, medicine.diagnostic_test, business.industry, SPG11, Spastic Paraplegia, Hereditary, Proteins, Magnetic resonance imaging, Original Articles, Phenotype, Magnetic Resonance Imaging, lcsh:Genetics, 030104 developmental biology, Autosomal Recessive Hereditary Spastic Paraplegia, Original Article, Female, ALS, business

Abstract

Background SPG11 mutations can cause autosomal recessive hereditary spastic paraplegia (ARHSP) and juvenile amyotrophic lateral sclerosis (JALS). Because these diseases share some clinical presentations and both can be caused by SPG11 mutations, it was considered that definitive diagnosis may not be straight forward. Methods The DNAs of referred ARHSP and JALS patients were exome sequenced. Clinical data of patients with SPG11 mutations were gathered by interviews and neurological examinations including electrodiagnosis (EDX) and magnetic resonance imaging (MRI). Results Eight probands with SPG11 mutations were identified. Two mutations are novel. Among seven Iranian probands, six carried the p.Glu1026Argfs*4‐causing mutation. All eight patients had features known to be present in both ARHSP and JALS. Additionally and surprisingly, presence of both thin corpus callosum (TCC) on MRI and motor neuronopathy were also observed in seven patients. These presentations are, respectively, key suggestive features of ARHSP and JALS. Conclusion We suggest that rather than ARHSP or JALS, combined ARHSP/JALS is the appropriate description of seven patients studied. Criteria for ARHSP, JALS, and combined ARHSP/JALS designations among patients with SPG11 mutations are suggested. The importance of performing both EDX and MRI is emphasized. Initial screening for p.Glu1026Argfs*4 may facilitate SPG11 screenings in Iranian patients., Nineteen patients of eight families with SPG11 mutations are described. Two previously unreported SPG11 mutations are reported. Definitive diagnosis of ARHSP or JALS is sometimes very difficult. Rather than ARHSP or JALS, combined ARHSP/JALS is the appropriate description for some patients with SPG11 mutation. Criteria for ARHSP, JALS, and combined ARHSP/JALS designations among patients with SPG11 mutations are suggested.

Published

2020

37. Bi-allelic Mutations in ALDH5A1 is associated with succinic semialdehyde dehydrogenase deficiency and severe intellectual disability

Author

Ahoura Nozari, Parisa Motamedian Dehkordi, Marzieh Javid, Ata Bushehri, Afagh Alavi, Saghar Ghasemi Firouzabadi, Farkhondeh Behjati, Javad Karimian, Vahid Asghariazar, Mahshid Fattahi, and Saeed Farajzadeh Valiliou

Subjects

0301 basic medicine, Succinic semialdehyde dehydrogenase deficiency, medicine.medical_specialty, Mutation, General Medicine, Biology, medicine.disease, medicine.disease_cause, Succinic semialdehyde, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, Endocrinology, chemistry, Autism spectrum disorder, 030220 oncology & carcinogenesis, Internal medicine, Anticipation (genetics), Intellectual disability, Genetics, medicine, Aldehyde dehydrogenase 5 family, member A1, Missense mutation

Abstract

Homozygous mutations of ALDH5A1 have been reportedly associated with Succinic semialdehyde dehydrogenase deficiency (SSADHD) that affects gamma-aminobutyric acid (GABA) catabolism and evinces a wide range of clinical phenotype from mild intellectual disability to severe neurodegenerative disorders. We report clinical and molecular data of a Lor family with 2 affected members presenting with severe intellectual disability, developmental delay, and generalized tonic-clonic seizures. A comprehensive genetic study that included whole-exome sequencing identified a homozygous missense substitution (NM_001080:c.G1321A:p.G441R) in ALDH5A1 (Aldehyde Dehydrogenase 5 Family Member A1) gene, consistent with clinical phenotype in the patients and co-segregating with the disease in the family. The non-synonymous mutation, p.G441R, affects a highly conserved amino acid residue, which is expected to cause a severe destabilization of the enzyme. Protein modeling demonstrated an impairment of the succinic semialdehyde (SSA) binding tunnel accessibility, and the anticipation of the protein folding stability and dynamics was a decrease in the free energy by 4.02 kcal/mol. Consistent with these in silico findings, excessive γ -hydroxybutyrate (GHB) could be detected in patients' urine as the byproduct of the GABA pathway. SSADHD, Succinic semialdehyde dehydrogenase deficiency; GABA, gamma-aminobutyric acid; ALDH5A1, Aldehyde Dehydrogenase 5 Family Member A1; GHB, γ -hydroxybutyrate; SSA, succinic semi aldehyde; WISC, Wechsler Intelligence Scale for Children; CNS, central nervous system ; EEG, electroencephalography; EEEF, empirical effective energy functions; ASD, autism spectrum disorder; ADHD, attention deficit hyperactivity disorder; IQ, intelligence quotient; EMG, electromyography; NCV, nerve conduction velocity; CP, cerebral palsy.

Published

2020

38. Whole-Exome Sequencing Identifies Three Candidate Homozygous Variants in a Consanguineous Iranian Family with Autism Spectrum Disorder and Skeletal Problems

Author

Farkhondeh Behjati, Saeed Farajzadeh Valilou, Susan Banihashemi, Seyed Gholamreza Noorazar, Fatemeh Hadipour, Mahshid Fattahi, Ahoura Nozari, Mahdiyeh Pashaei, Zahra Hadipour, Javad Karimian, Bijan Maghsoodlou Estrabadi, Afagh Alavi, Yousef Shafeghati, and Saghar Ghasemi Firouzabadi

Subjects

Genetics, Proband, Biology, medicine.disease, SNP genotyping, Developmental disorder, Neurodevelopmental disorder, Autism spectrum disorder, mental disorders, medicine, Autism, Original Article, Sibling, Genetics (clinical), Exome sequencing

Abstract

Autism spectrum disorder (ASD) is characterized by 3 core symptoms with impaired social communication, repetitive behavior, and/or restricted interests in early childhood. As a complex neurodevelopmental disorder (NDD), the phenotype and severity of autism are extremely heterogeneous. Genetic factors have a key role in the etiology of autism. In this study, we investigated an Azeri Turkish family with 2 ASD-affected individuals to identify probable ASD-causing variants. First, the affected individuals were karyotyped in order to exclude chromosomal abnormalities. Then, whole-exome sequencing was carried out in one affected sibling followed by cosegregation analysis for the candidate variants in the family. In addition, SNP genotyping was carried out in the patients to identify possible homozygosity regions. Both proband and sibling had a normal karyotype. We detected 3 possible causative variants in this family: c.5443G>A; p.Gly1815Ser, c.1027C>T; p.Arg343Trp, and c.382A>G; p.Lys128Glu, which are in the FBN1, TF, and PLOD2 genes, respectively. All of the variants cosegregated in the family, and SNP genotyping revealed that these 3 variants are located in the homozygosity regions. This family serves as an example of a multimodal polygenic risk for a complex developmental disorder. Of these 3 genes, confluence of the variants in FBN1 and PLOD2 may contribute to the autistic features of the patient in addition to skeletal problems. Our study highlights the genetic complexity and heterogeneity of NDDs such as autism. In other words, in some patients with ASD, multiple rare variants in different loci rather than a monogenic state may contribute to the development of phenotypes.

Published

2020

39. A novel nonsense mutation in WNK1/HSN2 associated with sensory neuropathy and limb destruction in four siblings of a large Iranian pedigree

Author

Fatemeh Fekrmandi, Afagh Alavi, Sareh Asadi, Abolhassan Ahmadiani, Behrouz Rahmani, Tannaz Ahadi, and Keivan Ahadi

Subjects

0301 basic medicine, Male, Nonsense mutation, Iran, lcsh:RC346-429, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, WNK Lysine-Deficient Protein Kinase 1, Hereditary sensory and autonomic neuropathy, HSN2, Medicine, Humans, HSAN2, Gene, Exome sequencing, lcsh:Neurology. Diseases of the nervous system, Hereditary sensory and autonomic neuropathies, Genetics, Sanger sequencing, business.industry, Siblings, General Medicine, medicine.disease, Pedigree, 030104 developmental biology, Codon, Nonsense, Whole exome sequencing, WNK1 gene, Mutation (genetic algorithm), symbols, Allelic heterogeneity, Female, Neurology (clinical), business, 030217 neurology & neurosurgery, Research Article

Abstract

Background Hereditary sensory and autonomic neuropathy type 2 (HSAN2) is an autosomal recessive disorder with predominant sensory dysfunction and severe complications such as limb destruction. There are different subtypes of HSAN2, including HSAN2A, which is caused by mutations in WNK1/HSN2 gene. Methods An Iranian family with four siblings and autosomal recessive inheritance pattern whom initially diagnosed with HSAN2 underwent whole exome sequencing (WES) followed by segregation analysis. Results According to the filtering criteria of the WES data, a novel candidate variation, c.3718C > A in WNK1/HSN2 gene that causes p.Tyr1025* was identified. This variation results in a truncated protein with 1025 amino acids instead of the wild-type product with 2645 amino acids. Sanger sequencing revealed that the mutation segregates with disease status in the pedigree. Conclusions The identified novel nonsense mutation in WNK1/HSN2 in an Iranian HSAN2 pedigree presents allelic heterogeneity of this gene in different populations. The result of current study expands the spectrum of mutations of the HSN2 gene as the genetic background of HSAN2A as well as further supports the hypothesis that HSN2 is a causative gene for HSAN2A. However, it seems that more research is required to determine the exact effects of this product in the nervous system.

Published

2018

40. Pantothenate kinase-associated neurodegeneration mimicking Tourette syndrome: a case report and review of the literature

Author

Mohammad Rohani, Mohammad-Masoud Rahimi Bidgoli, Alfonso Fasano, Leila Javanparast, Anthony E. Lang, Afagh Alavi, and Babak Zamani

Subjects

0301 basic medicine, medicine.medical_specialty, Neurology, business.industry, Dermatology, General Medicine, medicine.disease, Tourette syndrome, Pantothenate kinase-associated neurodegeneration, 03 medical and health sciences, Psychiatry and Mental health, 030104 developmental biology, 0302 clinical medicine, medicine, Neurology (clinical), Neurosurgery, business, Neuroscience, 030217 neurology & neurosurgery, Neuroradiology

Published

2018

41. A novel splicing variant in FLNC gene responsible for a highly penetrant familial dilated cardiomyopathy in an extended Iranian family

Author

Ehsan Aghaei-Moghadam, Mohammad-Taghi Majnoon, Reza Mollazadeh, Susan Banihashemi, Saghar Ghasemi Firouzabadi, Afagh Alavi, Akbar Mohammadzadeh, Mehrnoush Nikzaban, Ahoura Nozari, Farkhondeh Behjati, Hossein Najmabadi, and Aliakbar Zeinaloo

Subjects

Adult, Cardiomyopathy, Dilated, Male, 0301 basic medicine, Filamins, Haploinsufficiency, Iran, Biology, medicine.disease_cause, 03 medical and health sciences, Exon, Exome Sequencing, Genetics, medicine, Humans, Family, Genetic Predisposition to Disease, cardiovascular diseases, FLNC, Gene, Exome sequencing, Mutation, Splice site mutation, General Medicine, Middle Aged, Exon skipping, Nonsense Mediated mRNA Decay, Alternative Splicing, 030104 developmental biology, cardiovascular system, Female

Abstract

Recent achievements in the genetic diagnosis of Dilated Cardiomyopathy (DCM) have disclosed rare variants in numerous genes encoding different types of myocardial proteins. However, the causative gene underlying the pathogenesis of about 60% of familial cases with DCM has not been identified. One novel gene introduced in 2016 for cardiac-restricted DCM is FLNC. In this study, we applied Whole Exome Sequencing (WES) and bioinformatics-based methods to a member of an extended non-consanguineous family with DCM history accompanied with fatal arrhythmia in at least four consecutive generations. We found a novel splice-site mutation in FLNC gene (c.2389+1G>A) which cosegregated with all symptomatic individuals in the family. Computational prediction software tools as well as RT-PCR method were used to evaluate the impact of the FLNC splice site mutation. This substitution leads to exon 15th donor-site disruption and exon skipping, which would result in a premature stop codon three aminocids downstream of the mutation site. The aberrantly mRNA transcript can induce nonsense-mediated mRNA decay. Although carrier individuals show remarkable variable expression regarding the severity of DCM as well as the disease age of onset, a highly penetrant fatal arrhythmia was found to be shared between them. We strongly suggest that the involvement of FLNC gene, due to haploinsufficiency, should be considered in familial cases with DCM, especially if accompanied with arrhythmia and increased incidence of sudden cardiac death.

Published

2018

42. Beta-propeller protein associated neurodegeneration (BPAN); the first report of three patients from Iran with de novo novel mutations

Author

Gholam Ali Shahidi, Ghazal Haeri, Babak Zamani, Mohammad Rohani, Leila Javanparast, Fahimeh Haji Akhoundi, Anthony E. Lang, Alfonso Fasano, Mohammad Masoud Rahimi Bidgoli, and Afagh Alavi

Subjects

Beta-propeller, Neurology, Neurodegeneration with brain iron accumulation, Neurodegeneration, Cancer research, medicine, Neurology (clinical), Geriatrics and Gerontology, Biology, medicine.disease

Published

2019

43. Action Myoclonus and Seizure in Kufor‐Rakeb Syndrome

Author

Jose Bras, Alfonso Fasano, Anthony E. Lang, Mohammad Rohani, John Hardy, Elahe Elahi, Afagh Alavi, and Farzad Sina

Subjects

0301 basic medicine, Pediatrics, medicine.medical_specialty, business.industry, Neurodegeneration with brain iron accumulation, Nonsense mutation, Action myoclonus, nervous system diseases, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Neurology, Hypokinesia, Kufor Rakeb syndrome, Medicine, Case Series, Neurology (clinical), Spasticity, medicine.symptom, business, Myoclonus, 030217 neurology & neurosurgery, Exome sequencing

Abstract

Background Kufor-Rakeb syndrome (KRS) is a rare autosomal recessive neurologic disease with diverse phenotypic features. Herein we report an Iranian KRS family with seizure and action myoclonus in addition to other typical manifestations of this syndrome. Method All family members underwent careful neurologic examination. Exome sequencing was performed and ATP13A2 variation genotyped in all family members. Results Cognitive deficits, hypokinesia, rigidity, spasticity, brisk deep tendon reflexes, upward gaze palsy, tremor, and facial-faucial-finger mini-myoclonus were the common manifestations of all affected siblings. Two cases had seizure and the most severely affected sibling demonstrated severe action myoclonus. Exome sequencing identified a homozygous nonsense mutation c.2455C>T;p.Arg819* in ATP13A2 gene. Conclusions We reported five KRS affected siblings who manifested myoclonus and seizure. The most severely affected one demonstrated action myoclonus, which has not been reported so far.

Published

2017

44. The second mutation of SYCE1 gene associated with autosomal recessive nonobstructive azoospermia

Author

Hossein Najmabadi, Farzad Fatehi, Ramona Haji-Seyed-Javadi, Afagh Alavi, Mahdieh Pashaei, Davood Zare-Abdollahi, and Mohammad Masoud Rahimi Bidgoli

Subjects

0301 basic medicine, Infertility, Proband, Adult, Male, endocrine system, Hereditary spastic paraplegia, Biology, urologic and male genital diseases, Male infertility, 03 medical and health sciences, Consanguinity, Mice, 0302 clinical medicine, Exome Sequencing, medicine, Genetics, Animals, Humans, Genetic Predisposition to Disease, Central element, Genetics (clinical), Infertility, Male, Azoospermia, 030219 obstetrics & reproductive medicine, Splice site mutation, Homozygote, Obstetrics and Gynecology, General Medicine, medicine.disease, Pedigree, DNA-Binding Proteins, Synaptonemal complex, Meiosis, 030104 developmental biology, Reproductive Medicine, Codon, Nonsense, Mutation, RNA Splice Sites, Developmental Biology

Abstract

PURPOSE: It is estimated that 40–50% of infertility among human couples is due to male infertility. Azoospermia is estimated to occur in 1% of all men and to be the cause of 10–20% of male infertility. Genetic defects, including single gene effects, maybe cause of azoospermia in 20–30% of affected males. Here, we aim to identify the genetic cause of azoospermia in a man who is also affected by hereditary spastic paraplegia. METHODS: The proband was subjected to whole-exome sequencing, followed by a comprehensive in silico analysis to identify the azoospermia causative gene. RESULTS: A novel splice site mutation c.375-2A > G in SYCE1 that is thought to be the cause of azoospermia was identified. This variant co-segregated with azoospermia status in the family that has three additional affected males. CONCLUSION: SYCE1 gene encodes synaptonemal complex (SC) central element 1 protein which contributes to the formation of the synaptonemal complex during meiosis. Syce1 null male and female mice have been shown to be infertile. There have only been two reports on the effects of SYCE1 mutations in humans; it was shown as the cause of primary ovarian failure (POI) in one and as the cause of nonobstructive azoospermia (NOA) in another. We suggest that the mutation 375-2A > G, which affects the acceptor splice site within intron 6 of SYCE1, is the likely cause of azoospermia and subsequent infertility in the family studied. The finding constitutes the third report of SYCE1mutations that affect infertility in humans and further supports its contribution to this condition. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1007/s10815-019-01660-1) contains supplementary material, which is available to authorized users.

Published

2019

45. Late-Onset Mitochondrial Membrane Protein-Associated Neurodegeneration With Extensive Brain Iron Deposition

Author

Mahisa Mokhtari, Alfonso Fasano, Atefeh Davarzani, Mohammad Rohani, Afagh Alavi, Reza Hajati, and Anthony E. Lang

Subjects

Brain iron deposition, Pathology, medicine.medical_specialty, business.industry, Neurodegeneration with brain iron accumulation, Neurodegeneration, Late onset, medicine.disease, Revealing Images, Neurology, Mitochondrial Membrane Protein, Brain mri, medicine, Neurology (clinical), business

Published

2019

46. Continuum of phenotypes in hereditary motor and sensory neuropathy with proximal predominance and Charcot-Marie-Tooth patients with TFG mutation

Author

Shahriar Nafissi, Stephanie Efthymiou, Marzieh Khani, Hosein Shamshiri, Henry Houlden, Hanieh Taheri, Elahe Elahi, and Afagh Alavi

Subjects

0301 basic medicine, Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, Heterozygote, Neuromuscular disease, Adolescent, Gene Expression, Pedigree chart, 030105 genetics & heredity, Iran, medicine.disease_cause, 03 medical and health sciences, Charcot-Marie-Tooth Disease, Exome Sequencing, Genetics, medicine, Humans, Child, Genetics (clinical), Aged, Mutation, Base Sequence, business.industry, Infant, Proteins, Middle Aged, medicine.disease, Phenotype, Pedigree, 030104 developmental biology, Child, Preschool, Female, Hereditary motor and sensory neuropathy, business

Abstract

Charcot-Marie-Tooth (CMT) is a common neuropathy, and hereditary motor and sensory neuropathy with proximal predominance (HMSN-P) is a recently described rare neuromuscular disease. Although many genes have been implicated for CMT, TFG is the only known HMSN-P-causing gene. Within the framework of diagnostic criteria, clinical variation is evident among CMT-diagnosed and also HMSN-P-diagnosed individuals. Mutations that cause p.(Pro285Leu) and p.(Gly269Val) in TFG were earlier reported as cause of HMSN-P in two Iranian pedigrees. Here, we report the identification of p.(Gly269Val) in TFG as cause of CMT in a large Iranian pedigree. The clinical features of patients of the three pedigrees are presented and critically compared. Similarities between the two HMSN-P-diagnosed pedigrees with different TFG mutations, and differences between the two differentially diagnosed pedigrees with the same p.(Gly269Val) mutation were evident. The clinical features of the HMSN-P pedigree with the p.(Pro285Leu) and the CMT pedigree with the p.(Gly269Val) mutation were clearly congruent with the respective diagnoses, whereas the features of the HMSN-P-diagnosed pedigree with the p.(Gly269Val) were intermediate between the other two pedigrees. It is therefore suggested that the clinical features of the three Iranian pedigrees with TFG mutations and diagnosed with HMSN-P or CMT represent a continuum.

Published

2018

47. Tremor-Dominant Pantothenate Kinase-associated Neurodegeneration

Author

Alfonso Fasano, Anthony E. Lang, Mohammad Rohani, Afagh Alavi, Said Razme, Gholam Ali Shahidi, and Niloufar Yousefi

Subjects

Pathology, medicine.medical_specialty, medicine.diagnostic_test, Neurodegeneration with brain iron accumulation, Neurodegeneration, Biology, medicine.disease, PANK2, Pantothenate kinase-associated neurodegeneration, nervous system diseases, 030218 nuclear medicine & medical imaging, 03 medical and health sciences, 0302 clinical medicine, Neurology, Clinical diagnosis, Basal ganglia, medicine, Case Series, Neurology (clinical), Tremor dominant, 030217 neurology & neurosurgery, Genetic testing

Abstract

Background Neurodegeneration with brain iron accumulation (NBIA) includes rare and heterogeneous group of disorders characterized by iron deposition in the basal ganglia. Pantothenate kinase-associated neurodegeneration (PKAN), is the most common NBIA and has two main presentations: typical and atypical, the latter rarely presenting with tremor. Method Reported patients underwent full neurologic examination, a standard brain MRI and genetic testing for PKAN. Results Three cases of ‘tremor-dominant’ PKAN with a relatively benign course were reported: dystonic tremor was seen in one patient and Parkinsonian tremor in remaining ones. All of them had homozygous mutations in PANK2 gene and typical eye of the tiger sign on brain MRI. Conclusions PKAN (and NBIA in general) might be a potential cause of tremor, thus emphasizing the need to consider this diagnosis even in patients with a clinical diagnosis of essential, dystonic or Parkinsonian tremor. This article is protected by copyright. All rights reserved.

Published

2017

48. Genotype and phenotype analysis of 43 Iranian facioscapulohumeral muscular dystrophy patients; Evidence for anticipation

Author

Hossein Najmabadi, Afagh Alavi, Sara Esmaeili, Shahriar Nafissi, and Kimia Kahrizi

Subjects

musculoskeletal diseases, 0301 basic medicine, Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Weakness, Genotype, Chromosomal Proteins, Non-Histone, Genetic counseling, 030105 genetics & heredity, Iran, Genetic analysis, 03 medical and health sciences, 0302 clinical medicine, Genotype-phenotype distinction, Internal medicine, medicine, Facioscapulohumeral muscular dystrophy, Humans, Myopathy, Genetics (clinical), Homeodomain Proteins, business.industry, DNA Methylation, medicine.disease, Phenotype, Muscular Dystrophy, Facioscapulohumeral, Neurology, Pediatrics, Perinatology and Child Health, Anticipation (genetics), Mutation, Female, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Facioscapulohumeral muscular dystrophy (FSHD) is the third most common hereditary myopathy (prevalence 1/8300–1/20,000). It is typically characterized by progressive weakness of facial, scapular and humeral muscles. Pelvic, abdominal and lower limbs muscles may eventually be affected. FSHD is classified into two subgroups, FSHD1 and FSHD2. FSHD1 is due to a reduction in the copy number of D4Z4 macrosatellites on chromosome 4q35 (11–100 repeats in normal individuals and 1–10 repeats in patients), and FSHD2 is caused by mutations in SMCHD1 or DNMT3B. Here, we present clinical features and results of genetic analysis on 43 Iranian FSHD patients. Forty patients carried 2–7 D4Z4 repeats based on Southern blot analysis, thus confirming FSHD1 diagnosis in these patients. The number of patients with D4Z4 repeats in the range of 1–3, 4–6 and 7–9 were, respectively, 22, 17 and one. Patients with the lower number of D4Z4 repeats generally showed earlier onset and more severe disease presentations. Anticipation was observed in 14 multi-generational families. To the best of our knowledge, this is the first phenotype and genotype analysis of FSHD patients in the Iranian population. The results of this study will be beneficial for genetic counselling of FSHD patients and their families, and for the establishment of a simple affordable genetic test for Iranians as the majority of patients had 1–5 D4Z4 repeats.

Published

2017

49. LGMD2E is the most common type of sarcoglycanopathies in the Iranian population

Author

Gholamreza Zamani, Hossein Najmabadi, Afagh Alavi, Kimia Kahrizi, Fatemeh Jazayeri, Shahriar Nafissi, Sara Esmaeili, Seyed Hasan Tonekaboni, Yalda Nilipour, and Mahmoud Reza Ashrafi

Subjects

0301 basic medicine, Proband, Adult, Male, Adolescent, Biology, Iran, medicine.disease_cause, 03 medical and health sciences, Cellular and Molecular Neuroscience, SGCG, Young Adult, 0302 clinical medicine, Genetics, medicine, Sarcoglycanopathies, Humans, Multiplex ligation-dependent probe amplification, Child, Gene, SGCA, Retrospective Studies, Family Health, Mutation, 030104 developmental biology, Sarcoglycanopathy, Genetic Techniques, Haplotypes, Female, 030217 neurology & neurosurgery

Abstract

Sarcoglycanopathies (SGCs) which are caused by mutations in SGCA, SGCB, SGCG or SGCD genes are a subgroup of autosomal-recessive limb-girdle-muscular-dystrophies (LGMD2). Although frequencies of mutations in these genes are different among populations, mutations in SGCA and SGCD, respectively, have the highest and lowest frequencies in most populations. Here, we report the proportion of mutations in SGC genes among a group of Iranian SGCs patients. Clinical features and results of SGC genes screening of 25 SGCs probands are presented. Large deletion mutations are confirmed with MLPA assays. In total, 15 candidate disease causing mutations were observed in the SGCA, SGCB, SGCG and SGCD genes; ten were novel. Fourteen (56%), seven (28%), three (12%) and one (4%) patient, respectively, carried mutations in SGCB, SGCG, SGCD and SGCA. The findings suggest that LGMD2E is the most common form of SGCs in the Iranian population and that LGMD2D is the rarest. Twelve LGMD2E cases carried the same mutation. To the best of knowledge, the mutation spectrum in SGCs is being reported for the first time in Iranian population. The finding will be beneficial for screening and genetic-counseling of SGCs patients in Iran.

Published

2017

50. Mutations in C19orf12 and intronic repeat expansions in C9orf72 not observed in Iranian Parkinson's disease patients

Author

Maryam Malakouti Nejad, Afagh Alavi, Gholam Ali Shahidi, and Elahe Elahi

Subjects

Adult, Male, Aging, Parkinson's disease, Adolescent, Neurodegeneration with brain iron accumulation, Population, Disease, Biology, Iran, medicine.disease_cause, Bioinformatics, 050105 experimental psychology, Mitochondrial Proteins, 03 medical and health sciences, Young Adult, 0302 clinical medicine, C9orf72, medicine, Humans, 0501 psychology and cognitive sciences, Amyotrophic lateral sclerosis, education, Genetic Association Studies, Aged, Genetics, Aged, 80 and over, Mutation, education.field_of_study, DNA Repeat Expansion, C9orf72 Protein, General Neuroscience, Parkinsonism, 05 social sciences, Parkinson Disease, Middle Aged, medicine.disease, Introns, Female, Neurology (clinical), Geriatrics and Gerontology, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Various neurodegenerative disorders share some clinical features that sometimes renders differential diagnosis challenging. Genetic-based classification also has limitations as mutations in the same gene are sometimes associated with different clinically based diagnoses. In this light, we screened the C19orf12 neurodegeneration with brain iron accumulation (NBIA) causing gene and the C9orf72 intronic expansion mutation that is cause of amyotrophic lateral sclerosis in 186 Iranian Parkinson's disease (PD) patients. C19orf12 has previously been screened in PD patients in only one study, and to the best of our knowledge neither gene has ever been screened in a PD cohort from a Middle East population. The study was justified because mutations in C19orf12 had previously been shown to be common in Iranian neurodegeneration with brain iron accumulation patients and all the patients with mutations in this gene had exhibited Parkinsonism features. The C9orf72 intronic expansion mutation was screened because the mother of an Iranian amyotrophic lateral sclerosis patient with the expansion who had been diagnosed with PD also harbored the expansion. The screenings did not identify disease causing variations in either of the genes among the PD patients screened.

Published

2016